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超声分配器实现温和、快速、高效的晶体浸泡。

Gentle, fast and effective crystal soaking by acoustic dispensing.

机构信息

Diamond Light Source, Harwell Science and Innovation Campus, Didcot OX11 0DE, England.

Structural Genomics Consortium (SGC), University of Oxford, Oxford OX3 7DQ, England.

出版信息

Acta Crystallogr D Struct Biol. 2017 Mar 1;73(Pt 3):246-255. doi: 10.1107/S205979831700331X. Epub 2017 Mar 6.

Abstract

The steady expansion in the capacity of modern beamlines for high-throughput data collection, enabled by increasing X-ray brightness, capacity of robotics and detector speeds, has pushed the bottleneck upstream towards sample preparation. Even in ligand-binding studies using crystal soaking, the experiment best able to exploit beamline capacity, a primary limitation is the need for gentle and nontrivial soaking regimens such as stepwise concentration increases, even for robust and well characterized crystals. Here, the use of acoustic droplet ejection for the soaking of protein crystals with small molecules is described, and it is shown that it is both gentle on crystals and allows very high throughput, with 1000 unique soaks easily performed in under 10 min. In addition to having very low compound consumption (tens of nanolitres per sample), the positional precision of acoustic droplet ejection enables the targeted placement of the compound/solvent away from crystals and towards drop edges, allowing gradual diffusion of solvent across the drop. This ensures both an improvement in the reproducibility of X-ray diffraction and increased solvent tolerance of the crystals, thus enabling higher effective compound-soaking concentrations. The technique is detailed here with examples from the protein target JMJD2D, a histone lysine demethylase with roles in cancer and the focus of active structure-based drug-design efforts.

摘要

现代光束线的高通量数据收集能力不断扩大,这得益于 X 射线亮度的提高、机器人的容量以及探测器速度的提高,这使得瓶颈转移到了样品制备的上游。即使在使用晶体浸泡进行配体结合研究中,最能利用光束线能力的实验,主要限制因素仍然是需要温和且复杂的浸泡方案,例如逐步增加浓度,即使对于坚固且特征良好的晶体也是如此。在这里,描述了使用声滴喷射法对小分子进行蛋白质晶体浸泡的方法,结果表明,该方法对晶体非常温和,并且允许非常高的通量,在不到 10 分钟内可轻松完成 1000 个独特的浸泡。除了化合物消耗量非常低(每个样品数十纳升)外,声滴喷射的位置精度还能够将化合物/溶剂靶向放置在晶体之外并靠近液滴边缘,从而使溶剂逐渐扩散到液滴中。这不仅提高了 X 射线衍射的重现性,而且提高了晶体对溶剂的耐受性,从而能够实现更高的有效化合物浸泡浓度。本文详细介绍了该技术,并以 JMJD2D 蛋白靶标为例,JMJD2D 是一种组蛋白赖氨酸去甲基酶,与癌症有关,也是积极基于结构的药物设计工作的重点。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/8190/5349437/b7eb3ed4f424/d-73-00246-fig1.jpg

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